Reconciling the regulatory role of Munc18 proteins in SNARE-complex assembly

Rehman, Asma; Archbold, J.K.; Hu, Shuhong; Norwood, Suzanne J.; Collins, Brett M.; Martin, Jennifer L.

doi:10.1107/s2052252514020727

Cited by 14 publications

(7 citation statements)

References 55 publications

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“…Such flickers invariable end in no‐fusion, indicating that a substance needed to complete fusion is lacking . Such could be one of the proteins known to assist the SNARE complex in mediating fusion as discussed later. However, it has not been possible to identify the substance required, nor whether this is a specific problem for any particular granule subset.…”

Section: The Fusion Porementioning

confidence: 99%

“…The MUNC‐18 family regulates SNARE dependent fusion, but whether inhibitory to or supportive of fusion, has not been entirely clear. Consensus seems to dictate that the three known Munc‐18s are essential for fusion . Munc‐2 and Munc‐3 are present in peroxidase negative and peroxidase positive granules of neutrophils, respectively , but Munc‐18s are not known to dictate specificity of the interaction of the fusing partners.…”

Section: Control Of Degranulationmentioning

confidence: 99%

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Granulopoiesis and granules of human neutrophils

Cowland

Borregaard

2016

Immunological Reviews

291

340

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Granules are essential for the ability of neutrophils to fulfill their role in innate immunity. Granule membranes contain proteins that react to environmental cues directing neutrophils to sites of infection and initiate generation of bactericidal oxygen species. Granules are densely packed with proteins that contribute to microbial killing when liberated to the phagosome or extracellularly. Granules are, however, highly heterogeneous and are traditionally subdivided into azurophil granules, specific granules, and gelatinase granules in addition to secretory vesicles. This review will address issues pertinent to formation of granules, which is a process intimately connected to maturation of neutrophils from their precursors in the bone marrow. We further discuss possible mechanisms by which decisions are made regarding sorting of proteins to constitutive secretion or storage in granules and how degranulation of granule subsets is regulated.

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Section: The Fusion Porementioning

confidence: 99%

Section: Control Of Degranulationmentioning

confidence: 99%

Granulopoiesis and granules of human neutrophils

Cowland

Borregaard

2016

Immunological Reviews

291

340

View full text Add to dashboard Cite

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“…In mammals, the seven SM proteins act as syntaxin chaperones, targeting and directing the t-SNARES to form specific SNARE complexes [50, 51]. Platelets contain VPS33a and 33b, which are involved in dense and α-granule biogenesis, respectively [52, 53].…”

Section: Snare Regulatory Proteinsmentioning

confidence: 99%

The nuts and bolts of the platelet release reaction

Joshi

Whiteheart

2016

Platelets

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Secretion is essential to many of the roles that platelets play in the vasculature, e.g., thrombosis, angiogenesis, and inflammation, enabling platelets to modulate the microenvironment at sites of vascular lesions with a myriad of bioactive molecules stored in their granules. Past studies demonstrate that granule cargo release is mediated by Soluble NSF Attachment Protein Receptor (SNARE) proteins, which are required for granule-plasma membrane fusion. Several SNARE regulators, which control when, where, and how the SNAREs interact, have been identified in platelets. Additionally, platelet SNAREs are controlled by post-translational modifications, e.g., phosphorylation and acylation. Although there have been many recent insights into the mechanisms of platelet secretion, much still remains undefined. In this review, we focus on the mechanics of platelet secretion and discuss how the secretory machinery functions in the pathway leading to membrane fusion and cargo release.

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“…In fact, immunoprecipitation experiments and direct binding assays all appear to have excluded Munc18a as a likely partner for syntaxin4 (41, 65), despite the fact that Munc18a shows (slightly) stronger affinity for the N-peptide of syntaxin4 than that of syntaxin1 (66). Since detergent lysates or soluble domains of syntaxin4 were used in the majority of the binding studies, which might introduce unexpected artifacts (25), we decided to use full-length syntaxin4 anchored in lipid bilayers as an alternative platform in our binding assay. We incubated His 6 -tagged Munc18a with liposomes bearing either syntaxin3 or syntaxin4 overnight at 4°C.…”

Section: Resultsmentioning

confidence: 99%

Munc18a clusters SNARE-bearing liposomes prior to trans-SNARE zippering

Arnold

Adhikari

Kang

et al. 2017

Biochemical Journal

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Sec1-Munc18 (SM) proteins cooperate with SNAREs {SNAP [soluble NSF (N-ethylmaleimide-sensitive factor) attachment protein] receptors} to mediate membrane fusion in eukaryotic cells. Studies of Munc18a/Munc18-1/Stxbp1 in neurotransmission suggest that SM proteins accelerate fusion kinetics primarily by activating the partially zippered trans-SNARE complex. However, accumulating evidence has argued for additional roles for SM proteins in earlier steps in the fusion cascade. Here we investigate the function of Munc18a in reconstituted exocytic reactions mediated by neuronal and non-neuronal SNAREs. We show that Munc18a plays a direct role in promoting proteoliposome clustering, underlying vesicle docking during exocytosis. In the three different fusion reactions examined, Munc18a-dependent clustering requires an intact N-terminal peptide (N-peptide) motif in syntaxin that mediates the binary interaction between syntaxin and Munc18a. Importantly, clustering is preserved under inhibitory conditions that abolish both trans-SNARE complex formation and lipid mixing, indicating that Munc18a promotes membrane clustering in a step that is independent of trans-SNARE zippering and activation.

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Reconciling the regulatory role of Munc18 proteins in SNARE-complex assembly

Cited by 14 publications

References 55 publications

Granulopoiesis and granules of human neutrophils

Granulopoiesis and granules of human neutrophils

The nuts and bolts of the platelet release reaction

Munc18a clusters SNARE-bearing liposomes prior to trans-SNARE zippering

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